NICE Implementation Collaborative Supporting local implementation of NICE guidance on use of the novel (non-Vitamin K antagonist) oral anticoagulants in non-valvular atrial fibrillation
Endorsed by
NICE Implementation Collaborative
Supporting local implementation of NICE guidance on use of the non-Vitamin K antagonist oral anticoagulants (NOACs) in non-valvular atrial fibrillation This consensus report was developed following an initial workshop meeting at which health care professionals and patient group representatives discussed barriers to use of the non-Vitamin K antagonist oral anticoagulants (NOACs, previously called new or novel oral anticoagulants) for reducing stroke risk in non-valvular atrial fibrillation and how these barriers might be overcome locally to facilitate appropriate use of the drugs. The meeting was held on behalf of the NICE Implementation Collaborative, which provides support to the NHS to implement NICE technology appraisals.
Key Points • The three currently licensed NOACs – dabigatran, rivaroxaban and apixaban – have been approved by NICE as options for the prevention of stroke and systemic embolism in patients with non-valvular atrial fibrillation • The drugs must therefore be made available for prescribing within their licensed indications, and should be automatically included in local formularies • Local arrangements for use of antithrombotic therapies in atrial fibrillation should be reviewed and policies developed for integration of NOACs into the care pathway • The 2014 NICE clinical guideline on atrial fibrillation advises against use of aspirin for stroke prevention. Continued use of aspirin is a barrier to appropriate stroke prevention with oral anticoagulants • Key groups in whom NOACs should especially be considered include patients who cannot take vitamin K antagonists (VKAs), those who cannot be stabilised on VKAs with poor time in therapeutic range (e.g., <65%)
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despite adequate adherence, and those taking aspirin for stroke prevention • Patients must be actively involved with their clinician in decision making about their anticoagulant treatment options and agree the therapy that is best for them • As there is no need for routine coagulation monitoring with the NOACs, concern has been expressed about patient adherence. Health care professionals should ensure that patients understand why they are taking an anticoagulant for their atrial fibrillation and the expected benefits. Pharmacists can reinforce the importance of treatment each time they dispense patients’ prescriptions • There are, as yet, no specific antidotes for the NOACs but there are steps that can be taken to reverse the drugs’ effect in the event of a major bleed • Primary care prescribing of NOACs needs local leadership. Not all GPs can be expected to be expert in the area of anticoagulation for atrial fibrillation. As the epidemic of atrial fibrillation continues to increase, local anticoagulant “champions” will be needed to take the lead in this
NICE Implementation Collaborative
Consensus Group Martin R Cowie (chair), Professor of Cardiology, Imperial College London Sotiris Antoniou, Consultant Pharmacist for Cardiovascular Medicine, Barts Health NHS Trust Sue Bacon, Anticoagulation Nurse Specialist, Bristol Michael Carpenter, Consultant Geriatrician and Lead Stroke Physician, Wakefield Matthew Fay, General Practitioner, Bradford Raj Bilkhu, AF Association Beverley Hunt, Professor of Thrombosis and Haemostasis, Guy’s and St Thomas’ NHS Trust, London Eve Knight, Chief Executive, Anticoagulation Europe Gregory YH Lip, Professor of Cardiovascular Medicine, University of Birmingham Neal Maskrey, Consultant Clinical Adviser, Medicines and Prescribing Centre, NICE Terry McCormack, General Practitioner, Whitby Jo Roberts, General Practitioner, South Devon and Torbay Helen Williams, Consultant Pharmacist for Cardiovascular Disease, South London
THE NICE Implementation Collaborative was set up in 2012 to identify barriers to the implementation of NICE guidance, with the aim of ensuring that patients get quick and more consistent access to approved treatments. It is a partnership between the NHS, the life sciences industry, healthcare professional bodies, key health organisations and the public. The use of NOACs – dabigatran, rivaroxaban and apixaban – for stroke prevention in non-valvular atrial fibrillation (AF) is one of the key areas that the Collaborative is currently working on. To date there has been relatively low uptake of these drugs in England, particularly compared with other European countries.
Current guidance to the NHS in England on atrial fibrillation and the NOACs An updated NICE clinical guideline on the management of AF is published this month (June 2014).4 This replaces the 2006 clinical guideline, taking account of new evidence and the introduction of the NOACs. A related Quality Standard to define best practice is expected to be published in due course.
The importance of stroke prevention in atrial fibrillation Atrial fibrillation (AF) is the most common cardiac arrhythmia: It affects about 1.6% of the population in England.1 Men are more commonly affected than women and the prevalence of AF increases with age. AF is a major cause of ischaemic stroke, with the risk of stroke being five times higher than in a person with a normal heart rhythm.2 Anticoagulation to reduce the risk of stroke is an essential part of AF management but the Department of Health says that patients are not always appropriately anticoagulated. It suggests that 7,000 strokes could be avoided and 2,100 lives saved each year in England with appropriate AF management.3 3
NICE Implementation Collaborative
NICE technology appraisals have been issued for each of the currently licensed NOACs,5â&#x20AC;&#x201C;7 with all three drugs approved as options for the prevention of stroke and systemic embolism in non-valvular AF, within their licensed indications. The recommendations made in the technology appraisals are incorporated into the new clinical guideline. Current European guidance on AF is the European Society of Cardiology (ESC) guideline. This was published in 2010, with an update covering the new drugs in 2012.8,9
Funding arrangements for NICE-approved drugs It is a statutory obligation for commissioners to make funding available within three months for drugs that have been recommended by a NICE technology appraisal. This point was highlighted in a recent NICE Good Practice Guidance on developing and updating local formularies10 which says that drugs with a positive NICE technology appraisal should be automatically included within the local formulary. It emphasises that formularies should not duplicate NICE assessments or challenge an appraisal recommendation.
BARRIERS TO USE OF NOACS Use of aspirin for stroke prevention One of the barriers to appropriate use of anticoagulants in stroke prevention in AF is the myth about the superior safety of aspirin compared with vitamin K antagonists (VKAs). Aspirin was included in the 2006 NICE AF clinical guideline for use in certain situations. However, the evidence base has moved on. For example, the 2007 Birmingham Atrial Fibrillation Treatment of the Aged study (BAFTA)11 showed that for stroke prevention in AF patients aged â&#x2030;Ľ75 years there was no significant difference in major bleeding (or intracranial bleeding) risk between warfarin and aspirin. There has been a move away from aspirin in this indication because of its poor efficacy in reducing risk of stroke compared with the oral anticoagulants. In the new NICE clinical guideline,4 oral anticoagulants (a VKA or a NOAC) are recommended as first-line therapy for patients at increased stroke risk. NICE says that anticoagulation should be offered to people with a CHA2DS2VASc score of 2 or more, and considered for men with a CHA2DS2VASc score of 1, taking bleeding risk into account. The guideline emphasises that aspirin monotherapy should not be offered to patients for stroke prevention. Dual antiplatelet therapy (with aspirin and clopidogrel) might be considered if anticoagulation is contraindicated or not tolerated and the person has a CHA2DS2VASc score of 2 or above.
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National audit data for January – March 2013 from the Royal College of Physicians show that for patients with known AF admitted to hospital with stroke, only 36 per cent were taking an anticoagulant prior to admission and 38 per cent were taking antiplatelet drugs which the RCP comments “are considered ineffective for patients in AF.”12
Reversibility of effect Lack of reversibility is a frequently raised clinician objection to the NOACs. However, although there are, as yet, no specific antidotes for these drugs, there are steps that can be taken to reverse the drugs’ effect in the event of a major bleed. British guidelines on management of bleeding14 recommend cessation of treatment and general haemostatic measures. For minor bleeding, supportive measures, such as direct pressure, minor surgical intervention and fluid replacement, is recommended. In lifethreatening bleeding, pro-haemostatic agents such as Prothrombin Complex Concentrate (PCC) or activated Prothrombin Complex Concentrate (APCC) can be considered. Local protocols should be available on management of bleeding in patients taking oral anticoagulants. Cases of major bleeding are likely to increase as the drugs are used more widely. But it is important to note that in clinical trials all three NOACs were associated with reduced haemorrhagic stroke and intracerebral haemorrhage compared with warfarin.9 NICE has noted that intracerebral bleeding is the most feared bleeding outcome for patients taking anticoagulants.7 Recent reports of “real world” experience with dabigatran found that bleeding rates were consistent with the trial data.15,16
Cost issues Although cost is a perceived barrier to the use of NOACs, NICE has concluded that the drugs are cost-effective and must be available to patients within their licensed indications. Managed introduction of drugs can be useful, starting with the patient groups who are most likely to benefit. With NOACs, this would include patients who cannot take VKAs, those who cannot be stabilised on warfarin with
Current prescribing patterns in primary care For stroke risk stratification, the 2014 NICE AF guideline, and the ESC guideline, recommend use of CHA2DS2VASc rather than the original CHADS2 score. However, for the moment CHADS2 is still included in the Quality and Outcomes Framework indicator sets. One of the QOF indicators for atrial fibrillation is the percentage of patients with CHADS2 score >1 who are currently treated with anticoagulant. In 2012/13, 65% of patients in England received this intervention, but there is a high degree of exception reporting.13 Online data from 2,538 practices in England using the GRASP-AF audit tool show that, in October 2013, of patients with AF who had a CHADS2 score of ≥1, 46% were taking an anticoagulant and 35% were taking an antiplatelet agent.
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NICE Implementation Collaborative
poor time in therapeutic range (e.g., <65%4) and those taking aspirin for stroke prevention for whom a NOAC may be an option. Medical, societal and personal savings from avoiding stroke have to be taken into account.
The budgetary impact of NOAC introduction is demonstrated in the costing model shown in the Panel, which highlights the costs and benefits for specific patient groups.
A Costing Model for NOACs The drug acquisition cost (minus the cost of warfarin/INR monitoring) is highlighted for different patient groups together with the expected number of strokes that will be prevented for a CCG of population 300,000
= 10 strokes prevented
= up to 23 strokes prevented
= 22 strokes prevented (but most could be prevented with warfarin for £163k )
= 1 stroke prevented compared with warfarin
= 3 stroke prevented compared with warfarin
Modelled by Helen Williams Consultant Pharmacist for CVD, South London
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£238 K
£404 K
£542 K
£213 K
£594 K
Patients unable to take warfarin because of allergies/ CI and patients unable to comply with monitoring of warfarin (n=297)
Patients out of range (n=720)
Patients on aspirin or nothing (n=675)
New Patients (n=265)
Patients currently stable on warfarin (n=1,008)
CCG population 300,000 AF population = 4,800
NICE Implementation Collaborative
Assumptions and References Based on CCG population of 300,000; AF prevalence 1.6%1; AF population 4,800; assuming 75% require anticoagulation using CHA2DS2VASc score (n=3,600) and 75% uptake of anticoagulation in this cohort (n=2,700) • 11% patients unable to take warfarin because of allergies or contraindications or unable to comply with monitoring17 • 41.7% of patients fail to achieve ≥ 65% time within therapeutic range (TTR)18 • 25% patients on aspirin on nothing, assuming 75% uptake of warfarin • Annual new AF incidence rate 0.0886%
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• Cost of warfarin = £241 per annum; cost of novel oral anticoagulant = £803 per annum5 • Annual stroke event rate in untreated population = 5%20 • Warfarin reduces event rates by 64%21
Adherence Because the NOACs have predictable pharmacokinetics, coagulation control does not need to be monitored. This is convenient for both patients and health care professionals. However, with warfarin and the other VKAs the requirement for regular monitoring does have the benefit of re-inforcing to patients the importance of treatment and there is some concern that the lack of monitoring with the NOACs might lead to poor adherence. There is need for ongoing patient education and support. Health care professionals should ensure that patients understand why they are taking an anticoagulant and the expected benefits. Pharmacists can reinforce the importance of treatment and the need to take
every prescribed dose each time they dispense patients’ prescriptions. Good adherence is even more important with the NOACs than with VKAs because of the drugs’ relatively short half-lives. With warfarin, patients retain some benefit for 48–72 hours after missing a dose while with NOACs the anticoagulant effect fades rapidly after 12–24 hours.22 Programmes for patients to help support adherence may be available from the NOAC manufacturers.
LOCAL CARE PATHWAYS FOR USING NOACs NICE-approved treatments have to be made available for prescribing, but CCGs have flexibility in how to make this happen and different models will be used to suit local needs. Arrangements for use of antithrombotic therapies in atrial fibrillation should be reviewed and policies developed for integration of NOACs in the local care pathway. NICE guidance on introducing new medicines to a local formulary10 emphasises the importance of stakeholder engagement, communication and dissemination. There should be agreed protocols across primary and secondary care for initiation of NOAC therapy. There have been reports of patients being told they have to try a VKA first, before a NOAC can be considered. There should be no such restrictions and a NOAC can be considered for newly-diagnosed patients, for certain patients who are currently taking a VKA, and for patients currently taking aspirin.
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NICE Implementation Collaborative
In some cases CCGs might choose to commission a service from the hospital anticoagulant clinics. In primary care, not all GPs will want to take responsibility for the first prescription of a NOAC (although they should be familiar with the prescribing information). One approach could be for each practice to have a designated health care professional (GP, nurse or pharmacist) with expertise in the area of anticoagulation in AF to take the lead in this.
Local leadership In Bradford, Yorkshire, an AF Quality Improvement Programme demonstrates what can be achieved with local clinical leadership. The programme was set up to support practices wanting to increase their anticoagulant prescribing. Over 18 months, anticoagulant prescribing for patients with CHADS2 score ≥1 increased from 49% to 65% in practices taking part in the programme. Over 1,000 new patients were started on an anticoagulant, including high-risk patients who have in the past often only been given aspirin. In the lead GP’s practice, use of NOACs in patients with CHADS2 score ≥2 increased from 0% to 8.6% in the 18 months to October 2013. Patients taking warfarin who are compliant but have poor INR control are targeted for switching to a NOAC.
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NOAC hospital clinic In Buckinghamshire Healthcare NHS Trust, a pharmacist-led clinic in secondary care was set up to manage the entry of the NOACs, with active review and informed discussion and consideration of the anticoagulant options with patients.23 Except in an emergency, all NOACs are initiated in this clinic, with agreed criteria for use. Two weeks after the first prescription, patients have a follow-up telephone consultation to check on side effects and any anxieties. In most cases, patients are then discharged to the GP for continuation of prescribing. Preliminary feedback from patients and GPs has been positive. This model is seen as a successful collaboration between primary and secondary care for safe and cost-effective managed entry of the new drugs.
NICE Implementation Collaborative
AF clinics in secondary care: The Birmingham experience When stroke prevention is discussed with newly diagnosed VKA-naïve patients, patients are counselled on the need for oral anticoagulation and the pros and cons of antithrombotic therapy. Clinic staff routinely calculate the CHA2DS2-VASc and HAS-BLED scores to assess stroke and bleeding risk, respectively (as recommended in the NICE guideline4) and renal function (based on creatinine clearance). After seeing the doctor, the oral anticoagulant options are then discussed in an extra counselling session in the clinic conducted by a specialist nurse or psychologist. Indications, benefits and risks of oral anticoagulants are explained to patients, as well as the need for compliance. A checklist proforma is signed by the patient and counsellor. If the patient opts for warfarin, good quality anticoagulation control with TTR>70% is strongly emphasised. The availability of NOACs as an option is also discussed. In patients who are warfarin-naïve, a “trial of warfarin” is not undertaken, as such patients would be at risk of stroke during the initiation phase, while trying to achieve INR stability. The SAMeTT2R2* 24 score is used to help identify warfarin-naïve patients who are likely to do well on warfarin (SAMeTT2R2 score 0–1). Those who are predicted to do less well (SAMeTT2R2 score >2) are preferentially offered a NOAC. For patients already on warfarin, their TTR is assessed from their INRs on the computerised records or their anticoagulation booklet. In patients scheduled for cardioversion, a NOAC is the preferred option to enable early cardioversion, approximately three weeks after initiation of the NOAC. Extra counselling is performed to ensure that the patient fully understands the necessity for compliance as poor compliance would leave the patient unprotected against thromboembolism. A proforma is signed by the patient and counsellor, with emphasis on drug compliance pre- and post-cardioversion.
*SAMeTT2R2: : Sex female, Age <60 years, Medical history (at least 2 of the following – hypertension, diabetes, coronary artery disease/myocardial infarction, peripheral arterial disease, congestive heart failure, previous stroke, pulmonary disease, hepatic or renal disease), Treatment (interacting drugs (e.g., amiodarone for rhythm control): All 1 point. Plus current Tobacco use (2 points) and Race (non-Caucasian, 2 points)24
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NICE Implementation Collaborative
Shared decision making An essential part of appropriate prescribing of NOACs is to ensure that patients are fully informed and actively involved in decision making about their anticoagulant treatment. The NICE technology appraisals5–7 say: “The decision about whether to start treatment [with NOAC] should be made after an informed discussion between the clinician and the person about the risks and benefits [of NOAC] compared with warfarin [and the other NOACs]. For people who are taking warfarin, the potential risks and benefits of switching [to NOAC] should be considered in light of their level of International Normalised Ratio (INR) control.” NICE has emphasised25 that health care professionals have a duty to help patients
make decisions about their treatment “based on an understanding of the likely benefits and risks rather than on misconceptions” and must “accept that patients may have different views from healthcare professionals about the balance of risks, benefits and side effects of medicines.” For patients, key factors in favour of NOACs include quality of life benefits from removing the lifestyle restrictions and monitoring requirements associated with VKAs. But some patients will be reassured to have regular INR monitoring (and so may prefer warfarin), some might be concerned about the lack of a specific reversal agent and some might choose to have no anticoagulant therapy. The Panel shows examples of questions that patients might wish to ask when discussing anticoagulation.
Questions you may wish to ask your doctor about medicines26,27 What are the benefits of this medicine? What are the risks in using this medicine? What effect might the medicine have on my symptoms and everyday life? How long will it take to have an effect? Are there any side effects associated with this medicine? What other treatments are available? Will the medication I am taking be affected by other medication? Will food or drink affect my AF or medication? What if I miss a dose? How often will I need blood tests to check my blood thinning levels (INR)? [VKA only] Does the GP’s surgery offer INR testing, or where will I need to go for this? [VKA only] How often will I need to have a “check-up”? Who can I call if I feel more unwell than usual? How can I find out further information? Is there a local patient support group? What support can you offer me if I decide not to take any medicines?
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NICE Implementation Collaborative
Selecting appropriate patients for NOACs New patients NOACs might be prescribed for newlydiagnosed patients if this is the preferred option after discussion of the alternatives. Patients currently taking warfarin There will be some patients currently taking warfarin or other VKA for whom a switch to a NOAC is appropriate. These will include: • Patients who, despite adequate adherence, spend less than 65% of time in therapeutic range,4 indicating suboptimal anticoagulant control. • Patients with allergic reactions or intolerance to warfarin • Patients who have genuine difficulty in attending for INR monitoring Practical details on making the switch from warfarin are included in product SmPCs and in the EHRA guide.22 Patients currently taking aspirin Patients taking aspirin for stroke prevention are another priority group to consider. These patients can be directly switched from aspirin to a NOAC the next day.
Good practice points for patients taking a NOAC • After patients start on a NOAC, it is good practice for clinicians to see them for regular review, preferably every three months22 • Information on what to do when a dose is missed and on drug interactions (which are currently much fewer than with warfarin) is given in the product SmPCs • Rivaroxaban (at the dosage used for AF) should be taken with food as this increases its bioavailability. Absorption of dabigatran and apixaban is not affected by food • Patients should be encouraged to seek advice before taking over-the-counter medicines, including herbal remedies • Patients should be encouraged to carry an anticoagulant card for use in emergency situations. Several different cards are available, including the traditional “yellow card” but also a “green card” from the AF Association (www.atrialfibrillation.org.uk) or a NOAC card from the European Heart Rhythm Association (www.NOACforAF.eu). There is also a “medication passport” (www. clahrc-northwestlondon.nihr.ac.uk/ research-projects/bespoke-projects/mymedication-passport) • If a patient has a bleed and the NOAC is stopped, it is important to consider restarting the anticoagulant, after discussion with the patient, once the bleeding issue is resolved
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Renal function
Useful resources
As the NOACs are at least partially cleared by the kidney, there may be need for dose reduction in renal impairment. Patients with chronic kidney disease will need careful monitoring of renal function, with details of dose modifications in the product SmPCs and in the EHRA guide.22
AF Association http://www.atrialfibrillation. org.uk
Patients undergoing surgery There should be local protocols on when to stop a NOAC before elective surgery and invasive procedures, and when to restart the drug. “Bridging anticoagulation” is not generally necessary for planned surgery22 because of the drugs’ predictable decline in effect and rapid onset of action on restarting after surgery.
Practical guide The European Heart Rhythm Association (EHRA) has produced a practical guide to use of the NOACs in AF, covering a range of common clinical scenarios22
Non-valvular AF The NOACs are licensed for use in non-valvular AF. They must not be used in AF patients with rheumatic heart disease (including mitral stenosis) or metal heart valves.
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Anticoagulation Europe http://www. anticoagulationeurope.org Website developed by the European Heart Rhythm Association of the European Society of Cardiology http://www.afibmatters.org NICE. You and your prescribed medicines: Enabling and supporting patients to make informed decisions http://publications.nice. org.uk/ifp76 Making the most of your medicines: http:// www.rpharms.com/promoting-pharmacy-pdfs/ patients---making-the-most-of-medicines.pdf
More technical Practical guide for NOAC prescribing: www.NOACforAF.eu NICE. Medicines adherence: Involving patients in decisions about prescribed medicines and supporting adherence. Clinical Guideline 76; 2009. http://guidance.nice.org.uk/CG76 Centre for Pharmacy Postgraduate Education. Essential skills for medicines optimisation. http://www.cppe.ac.uk/learning/Details. asp?TemplateID=EssMedsOpt-E-01&Format=E &ID=115&EventID=43157 Guide on medicines optimisation http://www. rpharms.com/promoting-pharmacy-pdfs/ helping-patients-make-the-most-of-theirmedicines.pdf
NICE Implementation Collaborative
References 1. NICE. Support for commissioning: Anticoagulation therapy; May 2013. 2. NICE. Atrial fibrillation (update) final scope. http:// guidance.nice.org.uk/CG/Wave0/638/Scoping/ Scope/pdf/English 3. Department of Health. Cardiovascular Disease Outcomes Strategy. Improving outcomes for people with, or at risk of, cardiovascular disease. March 2013. 4. NICE. The management of atrial fibrillation. Clinical Guideline June 2014. 5. NICE. Dabigatran etexilate for the prevention of stroke and systemic embolism in atrial fibrillation. Technology Appraisal 249; 2012. 6. NICE. Rivaroxaban for the prevention of stroke and systemic embolism in people with atrial fibrillation. Technology Appraisal 256; 2012. 7. NICE. Apixaban for preventing stroke and systemic embolism in people with nonvalvular atrial fibrillation. Technology Appraisal 275; 2013. 8. Camm AJ, Kirchhof P, Lip GYH, et al, for the Task Force for the Management of Atrial Fibrillation of the European Society of Cardiology (ESC). Guidelines for the management of atrial fibrillation. Eur Heart J 2010;31:2369-429. 9. Camm AJ, Lip GYH. De Caterina R, et al. 2012 focused update of the ESC Guidelines for the management of atrial fibrillation. Eur Heart J 2012;33:2719-47. 10. NICE. Developing and updating local formularies. Good Practice Guidance 1; 2012. 11. Mant J, Hobbs FDR, Fletcher K, et al. Warfarin versus aspirin for stroke prevention in an elderly community population with atrial fibrillation (the Birmingham Atrial Fibrillation Treatment of the Aged Study, BAFTA): a randomised controlled trial. Lancet 2007;370:493 – 503. 12. Royal College of Physicans. Sentinel Stroke National Audit Programme (SSNAP). Clinical audit first pilot public report; August 2013. http://www.rcplondon. ac.uk/sites/default/files/ssnap_first_pilot_national_ report_january_-_march_2013_admissions_with_ appendices_.pdf 13. Health and Social Care information Centre. Quality and Outcomes Framework 2012–13. http://www.hscic.gov.uk/ 14. Makris M, Van Veen JJ, Tait CR, et al, on behalf of the British Committee for Standards in Haematology. Guideline on the management of bleeding in patients on antithrombotic agents. Br J Haematol 2012;160:35-46.
15. Southworth MR, Reichman ME, Unger EF. Dabigatran and postmarketing reports of bleeding. New Engl J Med 2013;368:1272-4. 16. Larsen TB, Rasmussen LH, Skjoth F, et al. Efficacy and safety of dabigatran etexilate and warfarin in “real-world” patients with atrial fibrillation. J Am Coll Cardiol 2013;61:2264-73. 17. Filippi A, Bettoncelli G, Zaninelli A. Detected atrial fibrillation in north Italy: Rates, calculated stroke risk and proportion of patients receiving anticoagulation therapy. Fam Pract 2000;17:337-9. 18. Connolly SJ, Pogue J, Eikelboom J, et al. Benefit of oral anticoagulation over antiplatelet therapy in atrial fibrillation depends on the quality of international normalized ratio control achieved by centres and countries as measured by time in therapeutic range. Circulation 2008;118:2029-37. 19. Murphy NF, Simpson CR, Jhund PS, et al. A national survey of the prevalence, incidence, primary care burden and treatment of atrial fibrillation in Scotland. Heart 2007:93:606-12. 20. Atrial Fibrillation investigators. Risk factors for stroke and efficacy of antithrombotic therapy in atrial fibrillation. Analysis of pooled data from five randomized controlled trials. Arch Intern Med 1994;154:1449-57. 21. Hart RG, Benavente O, McBride R, Pearce LA. Antithrombotic therapy to prevent stroke in patients with atrial fibrillation: A meta-analysis. Ann Intern Med 1999:131:492-501. 22. Heidbuchel H, Verhamme P, Alings M, et al. European Heart Rhythm Association Practical Guide on the use of new oral anticoagulants in patients with non-valvular atrial fibrillation. Europace 2013;15:625-51. 23. Bhandal S, Stapleton M, Ballinger J, et al. Managing the entry of a new therapeutic drug class in the Buckinghamshire area. Pharm J 2013;291:385-6. 24. Apostolakis S, Sullivan RM, Olshansky B, Lip GY. Factors affecting quality of anticoagulation control among patients with atrial fibrillation on warfarin: The SAMe-TT R score. Chest 2013;144:1555-63. 25. NICE. Medicines adherence. Involving patients in decisions about prescribed medicines and supporting adherence. Clinical Guideline 76; 2009. 26. AF Association. http://www.atrialfibrillation.org.uk/ files/file/Publications/120425-FINAL-Patient%20 and%20Primary%20Care%20Checklist.pdf 27. NICE. You and your prescribed medicines: enabling and supporting patients to make informed decisions. http://publications.nice.org.uk/you-and-yourprescribed-medicines-enabling-and-supportingpatients-to-make-informed-decisions-ifp76
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